Title of article
On the Solution Conformation and Dynamics of the HIV-1 Viral Infectivity Factor
Author/Authors
Sean R. Marcsisin، نويسنده , , Purushottam S. Narute، نويسنده , , Lori A. Emert-Sedlak، نويسنده , , Marek Kloczewiak، نويسنده , , Thomas E. Smithgall، نويسنده , , John R. Engen، نويسنده ,
Issue Information
روزنامه با شماره پیاپی سال 2011
Pages
15
From page
1008
To page
1022
Abstract
Human immunodeficiency virus-1 (HIV-1) has evolved a cunning mechanism to circumvent the antiviral activity of the APOBEC3 family of host cell enzymes. HIV-1 Vif [viral (also called virion) infectivity factor], one of several HIV accessory proteins, targets APOBEC3 proteins for proteasomal degradation and downregulates their expression at the mRNA level. Despite the importance of Vif for HIV-1 infection, there is little conformational data on Vif alone or in complex with other cellular factors due to incompatibilities with many structural techniques and difficulties in producing suitable quantities of the protein for biophysical analysis. As an alternative, we have turned to hydrogen exchange mass spectrometry (HX MS), a conformational analysis method that is well suited for proteins that are difficult to study using X-ray crystallography and/or NMR. HX MS was used to probe the solution conformation of recombinant full-length HIV-1 Vif. Vif specifically interacted with the previously identified binding partner Hck and was able to cause kinase activation, suggesting that the Vif studied by HX MS retained a biochemically competent conformation relevant to Hck interaction. HX MS analysis of Vif alone revealed low deuteration levels in the N-terminal portion, indicating that this region contained structured or otherwise protected elements. In contrast, high deuteration levels in the C-terminal portion of Vif indicated that this region was likely unstructured in the absence of cellular interacting proteins. Several regions within Vif displayed conformational heterogeneity in solution, including the APOBEC3G/F binding site and the HCCH zinc finger. Taken together, these HX MS results provide new insights into the solution conformation of Vif.
Keywords
APOBEC3F/G , Vif , Hydrogen exchange , mass spectrometry , E3 ligase
Journal title
Journal of Molecular Biology
Serial Year
2011
Journal title
Journal of Molecular Biology
Record number
1253945
Link To Document